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Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains

BACKGROUND: Plasmodium vivax is the most prevalent human malaria parasite, causing serious public health problems in malaria-endemic countries. Until recently the Duffy-negative blood group phenotype was considered to confer resistance to vivax malaria for most African ethnicities. We and others hav...

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Autores principales: Menard, Didier, Chan, Ernest R., Benedet, Christophe, Ratsimbasoa, Arsène, Kim, Saorin, Chim, Pheaktra, Do, Catherine, Witkowski, Benoit, Durand, Remy, Thellier, Marc, Severini, Carlo, Legrand, Eric, Musset, Lise, Nour, Bakri Y. M., Mercereau-Puijalon, Odile, Serre, David, Zimmerman, Peter A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3836732/
https://www.ncbi.nlm.nih.gov/pubmed/24278487
http://dx.doi.org/10.1371/journal.pntd.0002489
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author Menard, Didier
Chan, Ernest R.
Benedet, Christophe
Ratsimbasoa, Arsène
Kim, Saorin
Chim, Pheaktra
Do, Catherine
Witkowski, Benoit
Durand, Remy
Thellier, Marc
Severini, Carlo
Legrand, Eric
Musset, Lise
Nour, Bakri Y. M.
Mercereau-Puijalon, Odile
Serre, David
Zimmerman, Peter A.
author_facet Menard, Didier
Chan, Ernest R.
Benedet, Christophe
Ratsimbasoa, Arsène
Kim, Saorin
Chim, Pheaktra
Do, Catherine
Witkowski, Benoit
Durand, Remy
Thellier, Marc
Severini, Carlo
Legrand, Eric
Musset, Lise
Nour, Bakri Y. M.
Mercereau-Puijalon, Odile
Serre, David
Zimmerman, Peter A.
author_sort Menard, Didier
collection PubMed
description BACKGROUND: Plasmodium vivax is the most prevalent human malaria parasite, causing serious public health problems in malaria-endemic countries. Until recently the Duffy-negative blood group phenotype was considered to confer resistance to vivax malaria for most African ethnicities. We and others have reported that P. vivax strains in African countries from Madagascar to Mauritania display capacity to cause clinical vivax malaria in Duffy-negative people. New insights must now explain Duffy-independent P. vivax invasion of human erythrocytes. METHODS/PRINCIPAL FINDINGS: Through recent whole genome sequencing we obtained ≥70× coverage of the P. vivax genome from five field-isolates, resulting in ≥93% of the Sal I reference sequenced at coverage greater than 20×. Combined with sequences from one additional Malagasy field isolate and from five monkey-adapted strains, we describe here identification of DNA sequence rearrangements in the P. vivax genome, including discovery of a duplication of the P. vivax Duffy binding protein (PvDBP) gene. A survey of Malagasy patients infected with P. vivax showed that the PvDBP duplication was present in numerous locations in Madagascar and found in over 50% of infected patients evaluated. Extended geographic surveys showed that the PvDBP duplication was detected frequently in vivax patients living in East Africa and in some residents of non-African P. vivax-endemic countries. Additionally, the PvDBP duplication was observed in travelers seeking treatment of vivax malaria upon returning home. PvDBP duplication prevalence was highest in west-central Madagascar sites where the highest frequencies of P. vivax-infected, Duffy-negative people were reported. CONCLUSIONS/SIGNIFICANCE: The highly conserved nature of the sequence involved in the PvDBP duplication suggests that it has occurred in a recent evolutionary time frame. These data suggest that PvDBP, a merozoite surface protein involved in red cell adhesion is rapidly evolving, possibly in response to constraints imposed by erythrocyte Duffy negativity in some human populations.
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spelling pubmed-38367322013-11-25 Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains Menard, Didier Chan, Ernest R. Benedet, Christophe Ratsimbasoa, Arsène Kim, Saorin Chim, Pheaktra Do, Catherine Witkowski, Benoit Durand, Remy Thellier, Marc Severini, Carlo Legrand, Eric Musset, Lise Nour, Bakri Y. M. Mercereau-Puijalon, Odile Serre, David Zimmerman, Peter A. PLoS Negl Trop Dis Research Article BACKGROUND: Plasmodium vivax is the most prevalent human malaria parasite, causing serious public health problems in malaria-endemic countries. Until recently the Duffy-negative blood group phenotype was considered to confer resistance to vivax malaria for most African ethnicities. We and others have reported that P. vivax strains in African countries from Madagascar to Mauritania display capacity to cause clinical vivax malaria in Duffy-negative people. New insights must now explain Duffy-independent P. vivax invasion of human erythrocytes. METHODS/PRINCIPAL FINDINGS: Through recent whole genome sequencing we obtained ≥70× coverage of the P. vivax genome from five field-isolates, resulting in ≥93% of the Sal I reference sequenced at coverage greater than 20×. Combined with sequences from one additional Malagasy field isolate and from five monkey-adapted strains, we describe here identification of DNA sequence rearrangements in the P. vivax genome, including discovery of a duplication of the P. vivax Duffy binding protein (PvDBP) gene. A survey of Malagasy patients infected with P. vivax showed that the PvDBP duplication was present in numerous locations in Madagascar and found in over 50% of infected patients evaluated. Extended geographic surveys showed that the PvDBP duplication was detected frequently in vivax patients living in East Africa and in some residents of non-African P. vivax-endemic countries. Additionally, the PvDBP duplication was observed in travelers seeking treatment of vivax malaria upon returning home. PvDBP duplication prevalence was highest in west-central Madagascar sites where the highest frequencies of P. vivax-infected, Duffy-negative people were reported. CONCLUSIONS/SIGNIFICANCE: The highly conserved nature of the sequence involved in the PvDBP duplication suggests that it has occurred in a recent evolutionary time frame. These data suggest that PvDBP, a merozoite surface protein involved in red cell adhesion is rapidly evolving, possibly in response to constraints imposed by erythrocyte Duffy negativity in some human populations. Public Library of Science 2013-11-21 /pmc/articles/PMC3836732/ /pubmed/24278487 http://dx.doi.org/10.1371/journal.pntd.0002489 Text en © 2013 Menard et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Menard, Didier
Chan, Ernest R.
Benedet, Christophe
Ratsimbasoa, Arsène
Kim, Saorin
Chim, Pheaktra
Do, Catherine
Witkowski, Benoit
Durand, Remy
Thellier, Marc
Severini, Carlo
Legrand, Eric
Musset, Lise
Nour, Bakri Y. M.
Mercereau-Puijalon, Odile
Serre, David
Zimmerman, Peter A.
Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title_full Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title_fullStr Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title_full_unstemmed Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title_short Whole Genome Sequencing of Field Isolates Reveals a Common Duplication of the Duffy Binding Protein Gene in Malagasy Plasmodium vivax Strains
title_sort whole genome sequencing of field isolates reveals a common duplication of the duffy binding protein gene in malagasy plasmodium vivax strains
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3836732/
https://www.ncbi.nlm.nih.gov/pubmed/24278487
http://dx.doi.org/10.1371/journal.pntd.0002489
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